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We are analyzing https://link.springer.com/article/10.1007/bf00684996.

Title:
Chronic relapsing EAE time course of neurological symptoms and pathology | Acta Neuropathologica
Description:
The inflammatory reaction in chronic relapsing EAE was studied with special reference to the alterations found in the early stages of the disease (first attack, first remission, and first relapse). The inflammatory reaction during the early stages of the first attack was dominated by polymorphonuclear leukocytes, together with edema and sometimes hemorrhage, resembling the alterations found in hyperacute or neutrophilic EAE. The tissue reaction consisted of myelin, as well as axonal damage, and involved predominately the root entry zones and the subpial white matter in the lower thoracic and lumbo-sacral spinal cord, with less severe damage in grey and white matter in other regions of the brain. During the first remission, a variable amount of perivascular inflammatory cuffs of lymphocytes and mononuclear cells were found, but cellular infiltration into the neural parenchyma was confined to a few small perivascular areas. In the first relapse, a massive invasion of the neural parenchyma by mononuclear cells was noted, leading to large plaque-like zones of demyelination in the white matter. In this stage of the disease axonal damage was rare. The lesions were predominantly confined to the lower thoracic and lumbo-sacral spinal cord, but with increasing duration of the disease, higher portions of the spinal cord, as well as brain stem, cerebellar white matter, centrum semiovale and fornix were involved, too. Further relapses showed a similar pattern as described in the second attack, although in these animals lesions of different ages were always found. Parallel with the clinical observations, the inflammatory reaction in the central nervous system also diminished with the duration of the disease. A comparison between Strain 13 and Hartley guinea pigs revealed a more severe reaction during the first attack in the latter, possibly responsible for the high mortality of these animals during this stage of the disease.
Website Age:
28 years and 1 months (reg. 1997-05-29).

Matching Content Categories {πŸ“š}

  • Health & Fitness
  • Education
  • Telecommunications

Content Management System {πŸ“}

What CMS is link.springer.com built with?

Custom-built

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Traffic Estimate {πŸ“ˆ}

What is the average monthly size of link.springer.com audience?

🌠 Phenomenal Traffic: 5M - 10M visitors per month


Based on our best estimate, this website will receive around 5,000,019 visitors per month in the current month.
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How Does Link.springer.com Make Money? {πŸ’Έ}

The income method remains a mystery to us.

Not every website is profit-driven; some are created to spread information or serve as an online presence. Websites can be made for many reasons. This could be one of them. Link.springer.com has a secret sauce for making money, but we can't detect it yet.

Keywords {πŸ”}

google, scholar, encephalomyelitis, allergic, experimental, article, chronic, inflammation, exp, lesions, access, cell, neuropath, neurol, levine, privacy, cookies, content, acta, relapsing, eae, neurological, inflammatory, reaction, disease, white, matter, guinea, york, path, information, publish, research, search, lassmann, wisniewski, found, attack, hyperacute, spinal, cord, multiple, sclerosis, autoimmune, amer, mediated, immunity, proc, stone, data,

Topics {βœ’οΈ}

month download article/chapter chronic relapsing eae chronic autoimmune encephalomyelitis lumbo-sacral spinal cord related subjects chronic allergic encephalomyelitis full article pdf subpial white matter cerebellar white matter privacy choices/manage cookies experimental allergic encephalomyelitis multiple sclerosis autoimmune encephalomyelitis spinal cord pathological neutrophilic eae guinea pigs european economic area scope submit manuscript polymorphonuclear leukocytes small perivascular areas central nervous system human periodontal ligament repeated passive transfers migration inhibition factor nonspecific tissue injuries check access instant access basic research conditions privacy policy cell mediated immunity electron microscopic study electron microscopic studies white matter york state institute tissue reaction consisted perivascular inflammatory cuffs neurological signs occur accepting optional cookies root entry zones stem cells derived january 1978 volumeΒ 43 article log journal finder publish allergic encephalomyelitis article cite spinal cord localized forms article lassmann disease axonal damage acta neuropathol 43

Questions {❓}

  • Do neurological signs occur in experimental allergic encephalomyelitis in the absence of inflammatory lesions of the central nervous system?

Schema {πŸ—ΊοΈ}

WebPage:
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         headline:Chronic relapsing EAE time course of neurological symptoms and pathology
         description:The inflammatory reaction in chronic relapsing EAE was studied with special reference to the alterations found in the early stages of the disease (first attack, first remission, and first relapse). The inflammatory reaction during the early stages of the first attack was dominated by polymorphonuclear leukocytes, together with edema and sometimes hemorrhage, resembling the alterations found in hyperacute or neutrophilic EAE. The tissue reaction consisted of myelin, as well as axonal damage, and involved predominately the root entry zones and the subpial white matter in the lower thoracic and lumbo-sacral spinal cord, with less severe damage in grey and white matter in other regions of the brain. During the first remission, a variable amount of perivascular inflammatory cuffs of lymphocytes and mononuclear cells were found, but cellular infiltration into the neural parenchyma was confined to a few small perivascular areas. In the first relapse, a massive invasion of the neural parenchyma by mononuclear cells was noted, leading to large plaque-like zones of demyelination in the white matter. In this stage of the disease axonal damage was rare. The lesions were predominantly confined to the lower thoracic and lumbo-sacral spinal cord, but with increasing duration of the disease, higher portions of the spinal cord, as well as brain stem, cerebellar white matter, centrum semiovale and fornix were involved, too. Further relapses showed a similar pattern as described in the second attack, although in these animals lesions of different ages were always found. Parallel with the clinical observations, the inflammatory reaction in the central nervous system also diminished with the duration of the disease. A comparison between Strain 13 and Hartley guinea pigs revealed a more severe reaction during the first attack in the latter, possibly responsible for the high mortality of these animals during this stage of the disease.
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      headline:Chronic relapsing EAE time course of neurological symptoms and pathology
      description:The inflammatory reaction in chronic relapsing EAE was studied with special reference to the alterations found in the early stages of the disease (first attack, first remission, and first relapse). The inflammatory reaction during the early stages of the first attack was dominated by polymorphonuclear leukocytes, together with edema and sometimes hemorrhage, resembling the alterations found in hyperacute or neutrophilic EAE. The tissue reaction consisted of myelin, as well as axonal damage, and involved predominately the root entry zones and the subpial white matter in the lower thoracic and lumbo-sacral spinal cord, with less severe damage in grey and white matter in other regions of the brain. During the first remission, a variable amount of perivascular inflammatory cuffs of lymphocytes and mononuclear cells were found, but cellular infiltration into the neural parenchyma was confined to a few small perivascular areas. In the first relapse, a massive invasion of the neural parenchyma by mononuclear cells was noted, leading to large plaque-like zones of demyelination in the white matter. In this stage of the disease axonal damage was rare. The lesions were predominantly confined to the lower thoracic and lumbo-sacral spinal cord, but with increasing duration of the disease, higher portions of the spinal cord, as well as brain stem, cerebellar white matter, centrum semiovale and fornix were involved, too. Further relapses showed a similar pattern as described in the second attack, although in these animals lesions of different ages were always found. Parallel with the clinical observations, the inflammatory reaction in the central nervous system also diminished with the duration of the disease. A comparison between Strain 13 and Hartley guinea pigs revealed a more severe reaction during the first attack in the latter, possibly responsible for the high mortality of these animals during this stage of the disease.
      datePublished:
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